The miR-200–Zeb1 axis regulates key aspects of β-cell function and survival in vivo

The miR-200–Zeb1 axis regulates key aspects of β-cell function and survival in vivo

Objective: The miR-200–Zeb1 axis regulates the epithelial-to-mesenchymal transition (EMT), differentiation, and resistance to apoptosis. A better understanding of these processes in diabetes is highly relevant, as β-cell dedifferentiation and apoptosis contribute to the loss of functional β-cell mas...

Full description

Bibliographic Details
Main Authors: Alexandra C. Title, Pamuditha N. Silva, Svenja Godbersen, Lynn Hasenöhrl, Markus Stoffel
Format: Article
Language:English
Published: Elsevier 2021-11-01
Series:Molecular Metabolism
Subjects:
β-cell dedifferentiation
Epithelial-to-mesenchymal transition
Double-negative feedback loop
Islet aggregation
ER stress
microRNA
Online Access:http://www.sciencedirect.com/science/article/pii/S2212877821001125
id doaj-e229bf2c2f6941d39f712f934bc69355
record_format Article
spelling doaj-e229bf2c2f6941d39f712f934bc693552021-07-03T04:45:39ZengElsevierMolecular Metabolism2212-87782021-11-0153101267The miR-200–Zeb1 axis regulates key aspects of β-cell function and survival in vivoAlexandra C. Title0Pamuditha N. Silva1Svenja Godbersen2Lynn Hasenöhrl3Markus Stoffel4Institute of Molecular Health Sciences (IMHS), ETH Zürich, Otto-Stern-Weg 7, 8093, Zürich, Switzerland; Competence Center Personalized Medicine, ETH Zürich, Voltastrasse 24, 8044, Zürich, SwitzerlandInstitute of Molecular Health Sciences (IMHS), ETH Zürich, Otto-Stern-Weg 7, 8093, Zürich, SwitzerlandInstitute of Molecular Health Sciences (IMHS), ETH Zürich, Otto-Stern-Weg 7, 8093, Zürich, SwitzerlandInstitute of Molecular Health Sciences (IMHS), ETH Zürich, Otto-Stern-Weg 7, 8093, Zürich, SwitzerlandInstitute of Molecular Health Sciences (IMHS), ETH Zürich, Otto-Stern-Weg 7, 8093, Zürich, Switzerland; Competence Center Personalized Medicine, ETH Zürich, Voltastrasse 24, 8044, Zürich, Switzerland; Medical Faculty, University of Zürich, 8091, Zürich, Switzerland; Corresponding author. Institute of Molecular Health Sciences (IMHS), ETH Zürich, Otto-Stern-Weg 7, 8093, Zürich, Switzerland.Objective: The miR-200–Zeb1 axis regulates the epithelial-to-mesenchymal transition (EMT), differentiation, and resistance to apoptosis. A better understanding of these processes in diabetes is highly relevant, as β-cell dedifferentiation and apoptosis contribute to the loss of functional β-cell mass and diabetes progression. Furthermore, EMT promotes the loss of β-cell identity in the in vitro expansion of human islets. Though the miR-200 family has previously been identified as a regulator of β-cell apoptosis in vivo, studies focusing on Zeb1 are lacking. The aim of this study was thus to investigate the role of Zeb1 in β-cell function and survival in vivo. Methods: miR-200 and Zeb1 are involved in a double-negative feedback loop. We characterized a mouse model in which miR-200 binding sites in the Zeb1 3′UTR are mutated (Zeb1200), leading to a physiologically relevant upregulation of Zeb1 mRNA expression. The role of Zeb1 was investigated in this model via metabolic tests and analysis of isolated islets. Further insights into the distinct contributions of the miR-200 and Zeb1 branches of the feedback loop were obtained by crossing the Zeb1200 allele into a background of miR-141–200c overexpression. Results: Mild Zeb1 derepression in vivo led to broad transcriptional changes in islets affecting β-cell identity, EMT, insulin secretion, cell–cell junctions, the unfolded protein response (UPR), and the response to ER stress. The aggregation and insulin secretion of dissociated islets of mice homozygous for the Zeb1200 mutation (Zeb1200M) were impaired, and Zeb1200M islets were resistant to thapsigargin-induced ER stress ex vivo. Zeb1200M mice had increased circulating proinsulin levels but no overt metabolic phenotype, reflecting the strong compensatory ability of islets to maintain glucose homeostasis. Conclusions: This study signifies the importance of the miR-200–Zeb1 axis in regulating key aspects of β-cell function and survival. A better understanding of this axis is highly relevant in developing therapeutic strategies for inducing β-cell redifferentiation and maintaining β-cell identity in in vitro islet expansion.http://www.sciencedirect.com/science/article/pii/S2212877821001125β-cell dedifferentiationEpithelial-to-mesenchymal transitionDouble-negative feedback loopIslet aggregationER stressmicroRNA
collection DOAJ
language English
format Article
sources DOAJ
author Alexandra C. Title
Pamuditha N. Silva
Svenja Godbersen
Lynn Hasenöhrl
Markus Stoffel
spellingShingle Alexandra C. Title
Pamuditha N. Silva
Svenja Godbersen
Lynn Hasenöhrl
Markus Stoffel
The miR-200–Zeb1 axis regulates key aspects of β-cell function and survival in vivo
Molecular Metabolism
β-cell dedifferentiation
Epithelial-to-mesenchymal transition
Double-negative feedback loop
Islet aggregation
ER stress
microRNA
author_facet Alexandra C. Title
Pamuditha N. Silva
Svenja Godbersen
Lynn Hasenöhrl
Markus Stoffel
author_sort Alexandra C. Title
title The miR-200–Zeb1 axis regulates key aspects of β-cell function and survival in vivo
title_short The miR-200–Zeb1 axis regulates key aspects of β-cell function and survival in vivo
title_full The miR-200–Zeb1 axis regulates key aspects of β-cell function and survival in vivo
title_fullStr The miR-200–Zeb1 axis regulates key aspects of β-cell function and survival in vivo
title_full_unstemmed The miR-200–Zeb1 axis regulates key aspects of β-cell function and survival in vivo
title_sort mir-200–zeb1 axis regulates key aspects of β-cell function and survival in vivo
publisher Elsevier
series Molecular Metabolism
issn 2212-8778
publishDate 2021-11-01
description Objective: The miR-200–Zeb1 axis regulates the epithelial-to-mesenchymal transition (EMT), differentiation, and resistance to apoptosis. A better understanding of these processes in diabetes is highly relevant, as β-cell dedifferentiation and apoptosis contribute to the loss of functional β-cell mass and diabetes progression. Furthermore, EMT promotes the loss of β-cell identity in the in vitro expansion of human islets. Though the miR-200 family has previously been identified as a regulator of β-cell apoptosis in vivo, studies focusing on Zeb1 are lacking. The aim of this study was thus to investigate the role of Zeb1 in β-cell function and survival in vivo. Methods: miR-200 and Zeb1 are involved in a double-negative feedback loop. We characterized a mouse model in which miR-200 binding sites in the Zeb1 3′UTR are mutated (Zeb1200), leading to a physiologically relevant upregulation of Zeb1 mRNA expression. The role of Zeb1 was investigated in this model via metabolic tests and analysis of isolated islets. Further insights into the distinct contributions of the miR-200 and Zeb1 branches of the feedback loop were obtained by crossing the Zeb1200 allele into a background of miR-141–200c overexpression. Results: Mild Zeb1 derepression in vivo led to broad transcriptional changes in islets affecting β-cell identity, EMT, insulin secretion, cell–cell junctions, the unfolded protein response (UPR), and the response to ER stress. The aggregation and insulin secretion of dissociated islets of mice homozygous for the Zeb1200 mutation (Zeb1200M) were impaired, and Zeb1200M islets were resistant to thapsigargin-induced ER stress ex vivo. Zeb1200M mice had increased circulating proinsulin levels but no overt metabolic phenotype, reflecting the strong compensatory ability of islets to maintain glucose homeostasis. Conclusions: This study signifies the importance of the miR-200–Zeb1 axis in regulating key aspects of β-cell function and survival. A better understanding of this axis is highly relevant in developing therapeutic strategies for inducing β-cell redifferentiation and maintaining β-cell identity in in vitro islet expansion.
topic β-cell dedifferentiation
Epithelial-to-mesenchymal transition
Double-negative feedback loop
Islet aggregation
ER stress
microRNA
url http://www.sciencedirect.com/science/article/pii/S2212877821001125
work_keys_str_mv AT alexandractitle themir200zeb1axisregulateskeyaspectsofbcellfunctionandsurvivalinvivo
AT pamudithansilva themir200zeb1axisregulateskeyaspectsofbcellfunctionandsurvivalinvivo
AT svenjagodbersen themir200zeb1axisregulateskeyaspectsofbcellfunctionandsurvivalinvivo
AT lynnhasenohrl themir200zeb1axisregulateskeyaspectsofbcellfunctionandsurvivalinvivo
AT markusstoffel themir200zeb1axisregulateskeyaspectsofbcellfunctionandsurvivalinvivo
AT alexandractitle mir200zeb1axisregulateskeyaspectsofbcellfunctionandsurvivalinvivo
AT pamudithansilva mir200zeb1axisregulateskeyaspectsofbcellfunctionandsurvivalinvivo
AT svenjagodbersen mir200zeb1axisregulateskeyaspectsofbcellfunctionandsurvivalinvivo
AT lynnhasenohrl mir200zeb1axisregulateskeyaspectsofbcellfunctionandsurvivalinvivo
AT markusstoffel mir200zeb1axisregulateskeyaspectsofbcellfunctionandsurvivalinvivo
_version_ 1721321231652749312

Similar Items